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Recalcitrant Pharmaceuticals in the Aquatic Environment: A Comparative Screening Study of Their Occurrence, Formation of Phototransformation Products and Their in Vitro Toxicity

机译:水生环境中的顽固性药物:它们的发生,光转化产物的形成及其体外毒性的比较筛选研究

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摘要

Data allowing for a complete environmental risk assessment of pharmaceuticals and their photoderatives in the environment are still scarce. In the present study, in vitro toxicity and both bio- and photopersistence of various pharmaceuticals (aciclovir, allopurinol, cetirizine, cimetidine, fluconazole, hydrochlorothiazide, lisinopril, phenytoin, primidone, ranitidine, sotalol, sulpiride, tramadol and valsartane) as well as their phototransformation products were evaluated in order to fill data gaps and to help prioritise them for further testing. Twelve out of the fourteen compounds investigated were found to be neither readily nor inherently biodegradable in the Organisation of Economic Cooperation and Development-biodegradability tests. The study further demonstrates that the photo-induced transformation of the pharmaceuticals was faster upon irradiation with a Hg lamp (UV light) than with a Xe lamp emitting a spectrum that mimics sunlight. Comparing the non-irradiated with the respective irradiated solutions, a higher acute and chronic toxicity against bacteria was found for the irradiated solutions of seven compounds (cetirizine, cimetidine, hydrochlorothiazide, ranitidine, sulpiride, tramadol and valsartane). No cyto- and genotoxic effects were found in human cervical (HeLa) and liver (Hep-G2) cells for any of the investigated compounds or their phototransformation products. This comparative study documents that phototransformation products can arise as a result of UV treatment of wastewater containing these pharmaceuticals. It further demonstrates that some phototransformation products may have a higher environmental risk potential than the respective parent compounds because some phototransformation products exhibited a higher bacterial toxicity.
机译:尚缺乏用于对环境中的药物及其光衍生物进行完整的环境风险评估的数据。在本研究中,各种药物(阿昔洛韦,别嘌呤醇,西替利嗪,西咪替丁,氟康唑,氢氯噻嗪,赖诺普利,苯妥英钠,奎尼酮,雷尼替丁,雷诺替丁,舒必利,曲马多和缬沙坦)的体外毒性以及生物持久性和光敏性对光转化产品进行了评估,以填补数据空白并帮助确定它们的优先级以进行进一步测试。在经济合作与发展组织的生物可降解性测试中,被调查的十四种化合物中有十二种既不容易也不具有固有的生物降解性。这项研究进一步证明,用汞灯(紫外线)照射后,药物的光诱导转化要快于发射模拟太阳光谱的氙灯。将未辐照的溶液与相应的辐照溶液进行比较,发现对七种化合物(西替利嗪,西咪替丁,氢氯噻嗪,雷尼替丁,舒必利,曲马多和缬沙坦)的辐照溶液对细菌的急性和慢性毒性更高。对于所研究的任何化合物或其光转化产物,在人宫颈(HeLa)和肝(Hep-G2)细胞中均未发现细胞毒性和遗传毒性。这项比较研究证明,紫外线处理含有这些药物的废水会产生光转化产物。它进一步证明,某些光转化产物可能比相应的母体化合物具有更高的环境风险潜力,因为一些光转化产物表现出更高的细菌毒性。

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